Van Wauwe Jean, Haefner Burkhard
Department of Inflammation, Johnson & Johnson Pharmaceutical R&D, a Division of Janssen Pharmaceutica, Beerse, Belgium.
Drug News Perspect. 2003 Nov;16(9):557-65. doi: 10.1358/dnp.2003.16.9.829337.
Some 20 years ago, glycogen synthase kinase-3 (GSK-3) was categorized as one of several protein kinases that could phosphorylate glycogen synthase and regulate the glucose metabolism pathway. Today, GSK-3 is being identified as a ubiquitous serine/threonine protein kinase that participates in a multitude of cellular processes, ranging from cell membrane-to-nucleus signaling, gene transcription, translation, cytoskeletal organization to cell cycle progression and survival. Two functional aspects make GSK-3 a peculiar kinase: its activity is constitutive and downregulated after cell activation by phosphorylation or interaction with inhibitory proteins, and the enzyme prefers substrates that are specifically prepared, that is prephosphorylated, by other kinases. Its pleiotropic but unique activities have made GSK-3 a much sought-after target for the treatment of prevalent human diseases such as type 2 diabetes and Alzheimer's disease. Recent drug discovery efforts have identified small-molecule, orally active inhibitors of GSK-3. This accomplishment may represent the first step toward the development of novel therapeutic agents.
大约20年前,糖原合酶激酶-3(GSK-3)被归类为几种能够磷酸化糖原合酶并调节葡萄糖代谢途径的蛋白激酶之一。如今,GSK-3被确认为一种普遍存在的丝氨酸/苏氨酸蛋白激酶,它参与众多细胞过程,从细胞膜到细胞核的信号传导、基因转录、翻译、细胞骨架组织到细胞周期进程和存活。GSK-3作为一种特殊激酶有两个功能方面的特点:其活性是组成性的,在细胞通过磷酸化或与抑制蛋白相互作用而激活后被下调,并且该酶更喜欢由其他激酶特异性制备的底物,即预磷酸化的底物。其多效但独特的活性使GSK-3成为治疗诸如2型糖尿病和阿尔茨海默病等常见人类疾病备受追捧的靶点。最近的药物研发工作已经鉴定出GSK-3的小分子口服活性抑制剂。这一成果可能代表了开发新型治疗药物的第一步。
